首页> 美国卫生研究院文献>Elsevier Sponsored Documents >Antibody responses after intravaginal immunisation with trimeric HIV-1CN54 clade C gp140 in Carbopol gel are augmented by systemic priming or boosting with an adjuvanted formulation
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Antibody responses after intravaginal immunisation with trimeric HIV-1CN54 clade C gp140 in Carbopol gel are augmented by systemic priming or boosting with an adjuvanted formulation

机译:在Carbopol凝胶中用三聚体HIV-1CN54进化枝C gp140进行阴道内免疫后的抗体反应可通过全身性引发或佐剂制剂增强

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摘要

Optimum strategies to elicit and maintain antibodies at mucosal portals of virus entry are critical for the development of vaccines against human immunodeficiency virus (HIV). Here we show in non-human primates that a novel regimen of repeated intravaginal delivery of a non-adjuvanted, soluble recombinant trimeric HIV-1CN54 clade C envelope glycoprotein (gp140) administered in Carbopol gel can prime for B-cell responses even in the absence of seroconversion. Following 3 cycles of repeated intravaginal administration, throughout each intermenses interval, 3 of 4 macaques produced or boosted systemic and mucosally-detected antibodies upon intramuscular immunisation with gp140 formulated in AS01 adjuvant. Reciprocally, a single intramuscular immunisation primed 3 of 4 macaques for antibody boosting after a single cycle of intravaginal immunisation. Virus neutralising activity was detected against clade C and clade B HIV-1 envelopes but was restricted to highly neutralisation sensitive pseudoviruses.
机译:在病毒进入的粘膜入口诱导和维持抗体的最佳策略对于开发针对人类免疫缺陷病毒(HIV)的疫苗至关重要。在这里,我们在非人类灵长类动物中表明,在Carbopol凝胶中施用的非佐剂性,可溶性重组三聚体HIV-1CN54进化枝C包膜糖蛋白(gp140)的重复阴道内重复给药的新方案即使在不存在的情况下也可以引发B细胞反应血清转化。在重复3次重复阴道内给药后,在每个月经间隔内,用AS01佐剂配制的gp140进行肌内免疫后,每4只猕猴中的3只会产生或增强全身和粘膜检测抗体。相应地,一次阴道内免疫后,一次肌肉内免疫会引发4只猕猴中的3只增强抗体。可以检测到针对进化枝C和进化枝B的HIV-1包膜的病毒中和活​​性,但仅限于高度中和敏感的假病毒。

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